Malnutrition and Paediatric antiretroviral therapy - International AIDS

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Antiretroviral pharmacology in children: How malnutrition impacts

clinical management

Philippa Musoke MBChB, PhD Department of Paediatrics and Child Health School of Medicine, Makerere University, Kampala and MU-JHU Research Collaboration, Kampala Uganda

Prevalence of under nutrition in regions of the world, 2008

Malnutrition and HIV

• AIDS was recognized in Uganda as “slim disease” because of the severe wasting noted in infected adults

• Both stunting and wasting are common in infected

children • Children present with varying degrees of malnutrition

– 30-50% of children with severe acute malnutrition (SAM) are HIV infected

(Serwadda D et al 1985 , Bachou H et al. 2006, Doherty et al 2006 )

Definition of severe acute malnutrition

• Weight-for-height z score < - 3SD expected for age

• Mid upper arm circumference < 11.5 cm

• Weight-for-age z score < -3 SD = wasting

• Height-for-age z score < -3 SD = stunting

HIV infected children with malnutrition

• Non-edematous malnutrition more prevalent

• Associated micronutrient deficiencies – Vitamin A, iron, selenium and zinc

• Mortality higher despite nutritional rehabilitation

– 4 fold higher mortality when compared to uninfected children

• Initiation of antiretroviral therapy required to prevent

HIV disease progression

Fergusson P et al Trans R Soc Trop Med Hyg 2009

Mortality: severe acute malnutrition

• 220 Ugandan children hospitalized – Mortality of 24% ( 52 children died)

• 70% of the deaths occurred in the 1st week – Increased risk of death

• transfused or received IV fluids • 454 Malawi Cohort of children with SAM

– Overall mortality 14.8% – 35.45 HIV-infected vs 10.4% HIV-negative – Highest morality ( 75%) in those under 24 months

Bachou H et al BMC Pediatr 2006

Baseline characteristics: children initiating antiretroviral therapy

Baseline characteristics

30 Africa studies (n=100-4000)

MSF Cohort N=3936

Age years (median) 5 <5 (50% 1-3yrs)

CD4% (median) 6 -15% (53%<10%) 90%* WAZ (Weight-for-age z score)

- <2.0 - <2.0

HAZ (Height-for-age z score)

- <2.0 ND

Children started on ART: Older, lower CD4%, wasted and stunted

Sutcliffe CG et al Lancet Infect Dis 2008 ; Sauvagoet D et al Pediatr 2010

Severe immune suppression/age

Management of severe acute malnutrition • No complications : manage as out patient, use plumpy nut

• Complications: hospitalize and stabilize

– WHO ten step approach

• Stabilize with F75 milk – milk fortified with vitamins, electrolytes & micronutrients

(75kcal/100mls and 0.9g protein) – Antibiotics – Monitor for complications

• Rehabilitation phase – switch to F100 milk (100kcal/100mls) WHO recommends starting ART after nutritional stabilization

Response to antiretroviral therapy in severe acute malnutrition

An 8 year old female prior to ART and one year later (MUJHU)

WAZ and HAZ on antiretroviral therapy by treatment response

-2-1

01

2M

ean

waz

0 12 24 36 48Weeks of follow up

VS/IS VS/IFVF/IS VF/IF

-3-2

-10

12

Mea

n ha

z

0 12 24 36 48Weeks of follow up

VS/IS VS/IFVF/IS VF/IF

Figure 1b. Mean HAZ scores in the different treatment outcome groups during 48 weeks of HAART

Figure 1a. Mean WAZ scores in the different treatment outcome groups during 48 weeks of HAART

Note error bar type= 1standard error

Musoke P et al BMC Ped 2010

Response to antiretorviral therapy – UK vs Uganda

Kekitiinwa A et al JAIDS 2008

CD4% decline despite nutritional recovery in HIV infected children with SAM

Hughes SM et al. Pediatr 2009

Survival among Malnourished children started on HAART: Early and Late – 345 malnourished children

Follow-up time (days)

5004003002001000

Cum

Surv

ival

1.00

.95

.90

.85

.80

Time to HAART Start

Late: 10 + wks

Early: 0 - 10 wks

By one year only 6% of the children who started late would have died cf to 15% of those that started early

Kekitiinwa A et ak Abstract

National Paed HIV conference 2008, Uganda

Pharmacokinetic data of antiretroviral therapy in moderate

and severe malnutrition

Effect of Malnutrition on drug pharmacokinetics

• Disease states may affect PK by disrupting drug absorption, protein binding or metabolism.

• Severe malnutrition – reduced drug absorption

• villous atrophy of the intestinal lining • reduced gastric acidity

– low serum albumin • reduced binding of some drugs

• Diarrhoea and micronutrient deficiency impacts

absorption (Krishnaswamy K, Clin-Pharmacokinet 1989, Gilman RH Gastroentrol 1988)

Nevirapine drug levels in malnutrition

Pollack L et al J Antimicrob Chemotherapy

Normal nutrition wt for ht > 85%: Mild-moderate malnutrition wt for ht 70-85%

MEC MEC

MEC – minimum effective concentration = 3000ng/ml

N=25 N=12 NVP levels dependant on age and not degree of malnutrition

Nevirapine concentrations in Malawi and Zambian children on fixed dose combination

71 Malawian and 56 Zambian children Median age 8.4 vs 8.5 years Height for age: - 3.15 vs -1.84 Lower NVP concentrations: • Lower ht for age ( stunting) 0.37mg/ml per unit higher • Lower prescribed dose/m2 + 0.89 mg/ml per 50mg/m2 higher • Higher BMI for age (lack of wasting) - 0.42mg/ml per unit higher • Stunted children had lower NVP levels • Wasted children tended to have higher NVP levels

Ellis JC et al Antivir Ther 2007

Nevirapine (median and range) in children India

Swaminathan S et al J Antimicrobial Chemother 2011

Research Questions • What is the effect of severe acute malnutrition on the

pharmacokinetics of ARV drugs ?

• What is the most appropriate timing for initiation of ART in severe acute malnutrition ? – Would early or delayed initiation of ART reduce

mortality ?

• Would nutritional supplementation during ART initiation improve overall outcome ?

• Would supplementation of specific micronutrients improve outcome in those who are deficient ?

Research priorities identified at the WHO Guideline meeting (1-3 February 2012) to update WHO recommendations on

the management of children with severe malnutrition HIV-INFECTED CHILDREN WITH SEVERE ACUTE MALNUTRITION

• Establish PK characteristics of HIV-infected children being started on ART

• PK of other drugs incl. INH • The effectiveness (survival and complications) of early vs. late

initiation of ART • In HIV-infected children on ART to establish the relationship

between ART regimens including dosing and development of early complications such as acute malnutrition and oedema or later metabolic complications such as IRIS

• To determine the most effective therapeutic feeding approach for HIV infected children with SAM who have persistent diarrhoea

• To determine if the basic physiological abnormalities of HIV-infected children with SAM , with or without oedema, are the same as children with SAM without HIV and to describe significant differences

THANK YOU

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